Gambino’s
fatal Flu vaccine heart attack experience raises a profound question of
our vaccine safety methodology.It
takes ~6 weeks (or more) to develop immunity in a flu shot. Is it correct to
exclude fatal exacerbations of existing chronic infection conditions like heart
disease and COPD as vaccine-linked if they appear during the same ~6 week
immune system training period. I think not. If immune system is trained for
long-term sensitivity, the mistuning may be life-long. The causality is clear,
and the vaccine did it and it upsets the cause of death statistics in perverse
ways.

Of course vaccines with immune response adjuvants should not
be administered to chronically sick people. This is a rule that is too often
ignored.

How Vaccines Work

During the immune system training period of the vaccine, the
adjuvant is active, the immune system is excited, immune cells are being be
trained to recognize: vaccine (payload) components, vaccine contaminants,
chronic/latent infections, allergens, exotoxins, endotoxins, environmental
toxins, food molecules…. whatever is foreign and possibly also certain self-
molecules. The adjuvants train the immune system to recognize the targets, to
signal and to activate killer, phagocytes to attack targets and the mast cells
to make peroxides and other cell toxic molecules.

Tests of injection sites in France have shown that aluminum
adjuvants can stay in the arm muscle for years. As long as the adjuvant is in
your system you may keep training your immune system for new microbial
challenges.

Aluminum adjuvants are associated with persistent tissue toxicity
and Autoimmunity
Syndrome Induced by Adjuvants (ASIA)This provides chronic stimulation of ROS generation, locally
depleting (oxidizing) ascorbate in the tissues, or organs. Brain, Kidney,
Heart, Pancreas, arterial tissues.Plaques have traces of aluminum and copper that have been moved there by
macrophages.The localized ROS
in brain tissues depleting ascorbate is likely a main cause of loss of
biochemical functions in the generation of insulin in the pancreas and of
dopamine in the brain.Ascorbate is a
known electron donor for these reactions, so depletion of ascorbate can down
regulate the production of essential molecules. The effect of persistent
aluminum loading in the tissues is system wide and affects a myriad of
biochemical reactions.

How Vaccines Work With Infections

If you have an unstoppable chronic infection, you can train
the immune system to inflame in its presence, but the immune system may not be
able to overcome the infection. This is because ascorbate is depleted and
ascorbate plays a role in stopping infections, viral, bacterial, fungal,
protozoal.This leaves the vaccinated
host with lowered ascorbate and in a state of unending war and
inflammation.The vaccine promoters’
self-interest lies with denying any fault with the vaccine.As will be seen later, they have managed the
statistics to avoid blame and we do not even recognize that there is a problem.

Except now we have an Autism and Autism Spectrum Disability
epidemic of long-term development disorders. The probability of the disorder
was less than 1/4000 but it is now larger than 1/100, with no known way to stop
the multiple-caused trend, and it is getting worse.

Vitamin C Can Help Protect You

Vitamin C (ascorbic acid = AA), in small amounts, can quell
the inflammation, but it gets used up in the process. If you fail to replace
it, repeatedly, then the inflammation resumes. You now have a vitamin C
dependency that normal RDA amounts cannot satisfy, and the dietary authorities
take no notice of the fact that the RDA is not “one size fits all”. So the
medical authorities also ignore your and others’ special-needs; everyone must
look out for themselves and there is little normal way to get help.The more vaccinations during a lifetime the
more the immune system is hyped. There is no reset button.

One answer is to kill all the microbes, but this is
impossible in many cases.However, AA
in much higher microbe killing doses, in therapeutic formulations and with
appropriate dispensation protocols, can do this in more cases than are
recognized by medical authorities. See AA
pharmacokinetics.

Immune Functions and Inflammation

An elevation of immune functions produces more killed-cells
and endotoxins released when microbes die.Free blood AA is oxidized; AA blood levels fall to critical levels.
Histamine generation will increase exponentially as AA levels fall; toxemia
levels from the chronic latent infection conditions will rise; all these will
deplete the ascorbate levels in the blood and in the storage tissues. Rapid
onset scurvy (anascorbemia) is the result.

Adjuvants train immune cells to react to chronic infection
microbes (and the vaccine payload) in hyper-inflammatory ways. Persistent
chronic infections create persistent inflammation conditions. This hyper
inflammation accelerates the AA depletion and creates a high level AA intake
dependency.Normal AA in diet is
inadequate.AA depletion accelerates if
large and frequent new AA is not eaten.

A Family Case History of Flu Vaccine with Chronic Infections

We have personally seen this happen to a
135 pound 90 year old female family member with COPD and chronic UTIs.

A few weeks after the flu shot, systemic (all over muscle)
pains, feelings of sickness, and severe plantar fasciitis pain flares were
observed as separate episodes.All of these
symptoms greatly diminished and all pain ended, eliminated in less than 6
hours, when 2 grams of AA were consumed every 2-3 hours.Then without effective antibiotics for a
chronic UTI and a plugged urethra, inflammation flared. Cipro for the UTI without
ARBs induced toxemia and more pains and discomforts, again controlled by a
higher frequency of AA intake.

But the high level of AA was not consistently maintained on
a regular 24-hour basis. There were times with no AA intake for many sleeping
hours.

The half lifetime for blood AA is given in a PubMed article
as ˝ hour.This rule of thumb is used
below as a way to estimate possible rates and amounts of AA
depletion.

The First Major Incident: AA Depletion (again)

Forgetting to take AA at bedtime (9 pm) and arising (7am)
was a 10-hour period of no AA intake. A mild COPD exacerbation without
accompanying heart distress but with multiple whole body pains judged severe
was induced by AA levels dropping by factor of [ ˝]20 = 0.000001. A
visit to the hospital and IV Cipro for the UTI accompanied by AA as needed to
control overall pain and sickness-feeling left the patient feeling well by 5 PM
and she was released to return home.By
evening, she was feeling very well and energetic, after about 16 grams of AA
intake that day. CoQ10 intake was 30 mg per day.

The Second Major Incident: AA Depletion and a Heart Attack

Again, forgetting to take AA at bedtime (9 pm) and arising
(7am) was a 10 hour period of no AA intake. A severe COPD exacerbation occurred
with accompanying congestive heart pains, (fibrillation) and breathing
distress. Hypothetical AA levels would havedropped by factor of [ ˝]20 = 0.000001.

3 grams of AA were administered with 50 mg CoQ10. 911 was
called. ˝ hour after the first AA was given a slight improvement in condition
was observed.In-hospital treatment
included IV Cipro, other IV antibiotics, ARB cytokine cascade blockers, and
oxygen.

The family made sure she ate vitamin C: 2-3 grams whenever
she felt bad or had a coughing fit. The AA helped quell urge to cough within ˝
hour each time.Estimated daily AA
intake was about 16-24 grams AA per day while on the IV antibiotic to control
resulting toxemia from microbial die off.

She was in hospital for 6 days.On release her oxygen was borderline ~86%She was weak, needed oxygen, and had low
energy. Bladder still distended, persistent difficulty passing urine. No
urethra scopy performed in hospital.

She was instructed to take vitamin C, 2 grams at bedtime and
when arising and any time at night she had to urinate.CoQ10, 100 mg per day improved energy levels
considerably. AA, 2 grams more than 6 times per day.After 1 week no need for daily oxygen, only at night.Daytime O2 level had risen to 96%.For several days was able to walk unassisted
with walker for about ˝ mile each day on level surface with no oxygen. On
return home O2 level was 97%.Feeling
very energetic; enough to do housework and floor mopping.

Summary:

Flu shot with chronic infections (COPD and UTI) caused
vitamin C dependency of over 10 grams per day needed to control an increasing
inflammation state, followed 3 weeks later, by two major bouts of inflammation
exacerbations, COPD respiratory flare and heart inflammation with heart lung congestion
(COPD exacerbation) and also from the toxins of the UTI antibiotic microbe die
off.(same tissue sensitivities heart
circulatory tract cells and urinary tract epithelium)

Recovery of vitality was rapid if enough AA was eaten every
few hours.

This could have been the Gambino case, where flu shot caused
heart attack and death. Without AA supplementation the heart failure would have
been fatal.The AA and CoQ10 plus the
ARBs helped reduce the heart damage.The Cipro and other antibiotics temporarily stopped the UTI.The COPD is still there and it flares if AA
dosage or frequency is interrupted.Chronic coughs go away1/2 hour after several grams of AA are eaten.

Vaccine Epidemiology Methodology Issues:

It appears that the epidemiology of vaccine related
conditions is being managed.Statistics
events are edited out to minimize vaccine to adverse-incident linkages.By restricting the vaccine-related adverse-event
window to 3-4 days, the vaccine is excluded as a cause of later vaccine caused
sensitivities and adverse events.Vaccines have repeatedly been seen to train immune system of a
susceptible minority to respond aggressively, making them hyper allergic to
reinfection.In the past such vaccines
have been judged to dangerous to deploy.Now by editing the statistics, we approve dangerous vaccines.But we can also use the same adverse-event
exclusion rules to disprove valid claims.

Vaccinations change the death statistics causes from flu to
heart disease.Vaccination reduces the
flu deaths but it does so by increasing the number of earlier heart disease
deaths.After more and more
vaccinations, death from inflammation, as AA depletes, is more certain and
sooner.Flu infections responsesafter vaccination are expected to be more
moderate for well persons.For
chronically sick persons Flu vaccinations willtrain some persons to have severe inflammatory episodes.Flu death statistics look better for the
herd with the vaccine. Overall Flu death rates are decreased.

Faster Die-off of the Elderly and Infirm?

Net result is a slightly faster die off of the
(older/child/weak)chronically-infected
population and those with latent endotoxin loads.Causes of this die- off are sudden deaths: heart attacks, more
COPD exacerbations, SIDS, SBS, etc, caused by ascorbic acid depletion or rapid
onset scurvy.

Australian Dr Archie Kalokerinos’sbook Every Second Childshowed death rate fromanascorbemia after vaccinations was 50%in ~3 weeks.

Our family case history is Kalakorinos’ experience all over
again, except for an older person.Kalokerinos recommended AA supplementation at higher than RDA amounts
and the vaccine mass deaths stopped.Years later, in Uganda, the WHO vaccination programs were plagued by
mass deaths. Kalokerinos’s 1974 book was long forgotten.

The warnings on not giving vaccines to sick children should
be extended to the aged, infirm, COPD, heart conditions, UTI infections,
etc.

Do not vaccinate them;do not vaccinate them repeatedly; do not vaccinate them many at a time.
Vaccinate them and you make them more and more ascorbate dependent and you
increase their death rate overall.

Kalokerinos’s Lesson:

If vitamin C nutrition is inadequate, or a dependency
exists, vaccines
are very unsafe for a few.Sick
persons with gut, respiratory, heart/circulatory,
urinary, ear or other chronic infections should not be vaccinated; this is the
standard of good practice (for children) that is too often ignored by oblivious
clinicians.

Kalokerinos’s Warning:

Do an orthomolecular nutrition work up and an AA
assessmentbefore vaccinations.Vitamin C, in therapeutic doses, should be
administered before, during and for several weeks after vaccinations to improve
the success and reduce the risks of the vaccination-induced inflammation.

Kalokerinos’ lesson and his warning are almost universally
ignored.

Malpractice?; lawsuit!

Copyright KF and KM Poehlmann, January 2013, all rights reserved.

Our Experience and Qualifications

Inflammation,
chronic infections, nutrition and immunity are topics we have researched
broadly in our studies of worldwide medical knowledge, documented on the
Internet and in the historical archives of medicine.We have spent over ten calendar years reading about these
inter-related subjects, attending postgraduate medical conferences. We have
read countless medical texts, abstracts, papers, online in the National Library
of Medicine and contained at various authoritative medical, nutritional and
biological websites. The mass of the available information worldwide is
tremendous. Search engines can reach much of it, so it can be correlated
productively.

Disclaimer

Nothing herein or referenced herein should be considered prescriptive
for any medical condition.This
information is for study and education purposes only.The readers are advised to find and consult well-educated,
trained and licensed medical and nutritional practitioners who shall evaluate
the many circumstances and conditions of each of their patients and will devise
appropriate treatments and nutritional plans for them.It is recognized that each person has the
right and duty to be well informed about the best foods, nutrition and medical
practices available that will promote their own good health.The opinions expressed herein are those of
the author(s) and the sources cited and there are many divergences of opinions
on many topics. The readers must resolve the conflicts, in their own minds,
after careful consideration of all the details and after any further necessary
research and study.

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